SARS-CoV-2疫苗BBV152(COVAXIN®)和ChAdOx1 nCoV-19(COVISHIELD™)在印度血清阴性和血清阳性个体中的免疫原性:一项多中心、非随机观察性研究。
Immunogenicity of SARS-CoV-2 vaccines BBV152 (COVAXIN®) and ChAdOx1 nCoV-19 (COVISHIELD™) in seronegative and seropositive individuals in India: a multicentre, nonrandomised observational study.
作者信息
Asokan Mangaiarkarasi S, Joan Roshni Florina, Babji Sudhir, Dayma Girish, Nadukkandy Prajitha, Subrahmanyam Vinutha, Pandey Archana, Malagi Girish, Arya Pooja, Mahajan Vibhuti, Bhavikatti Jayateerth, Pawar Ketakee, Thorat Aishwarya, Shah Priyanki, Goud Ramakrishna B, Roy Bishnudeo, Rajukutty Shon, Immanuel Sushil, Agarwal Dhiraj, Saha Sankhanil, Shivaraj Akshatha, Panikulam Patricia, Shome Rajeshwari, Gulzar Shah-E-Jahan, Sharma Anusmrithi U, Naik Ajinkya, Talashi Shruti, Belekar Madhuri, Yadav Ritu, Khude Poornima, V Mamatha, Shivalingaiah Sudarshan, Deshmukh Urmila, Bhise Chinmayee, Joshi Manjiri, Inbaraj Leeberk Raja, Chandrasingh Sindhulina, Ghose Aurnab, Jamora Colin, Karumbati Anandi S, Sundaramurthy Varadharajan, Johnson Avita, Ramesh Naveen, Chetan Nirutha, Parthiban Chaitra, Ahmed Asma, Rakshit Srabanti, Adiga Vasista, D'souza George, Rale Vinay, George Carolin Elizabeth, John Jacob, Kawade Anand, Chaturvedi Akanksha, Raghunathan Anu, Dias Mary, Bhosale Anand, Raghu Padinjat, Shashidhara L S, Vyakarnam Annapurna, Bal Vineeta, Kang Gagandeep, Mayor Satyajit
机构信息
Christian Medical College, Vellore, Tamil Nadu, India.
National Centre for Biological Sciences, Bengaluru, Karnataka, India.
出版信息
Lancet Reg Health Southeast Asia. 2024 Feb 27;22:100361. doi: 10.1016/j.lansea.2024.100361. eCollection 2024 Mar.
BACKGROUND
There are limited global data on head-to-head comparisons of vaccine platforms assessing both humoral and cellular immune responses, stratified by pre-vaccination serostatus. The COVID-19 vaccination drive for the Indian population in the age group 18-45 years began in April 2021 when seropositivity rates in the general population were rising due to the delta wave of COVID-19 pandemic during April-May 2021.
METHODS
Between June 30, 2021, and Jan 28, 2022, we enrolled 691 participants in the age group 18-45 years across four clinical sites in India. In this non-randomised and laboratory blinded study, participants received either two doses of Covaxin® (4 weeks apart) or two doses of Covishield™ (12 weeks apart) as per the national vaccination policy. The primary outcome was the seroconversion rate and the geometric mean titre (GMT) of antibodies against the SARS-CoV-2 spike and nucleocapsid proteins post two doses. The secondary outcome was the frequency of cellular immune responses pre- and post-vaccination.
FINDINGS
When compared to pre-vaccination baseline, both vaccines elicited statistically significant seroconversion and binding antibody levels in both seronegative and seropositive individuals. In the per-protocol cohort, Covishield™ elicited higher antibody responses than Covaxin® as measured by seroconversion rate (98.3% vs 74.4%, p < 0.0001 in seronegative individuals; 91.7% vs 66.9%, p < 0.0001 in seropositive individuals) as well as by anti-spike antibody levels against the ancestral strain (GMT 1272.1 vs 75.4 binding antibody units/ml [BAU/ml], p < 0.0001 in seronegative individuals; 2089.07 vs 585.7 BAU/ml, p < 0.0001 in seropositive individuals). As participants at all clinical sites were not recruited at the same time, site-specific immunogenicity was impacted by the timing of vaccination relative to the delta and omicron waves. Surrogate neutralising antibody responses against variants-of-concern including delta and omicron was higher in Covishield™ recipients than in Covaxin® recipients; and in seropositive than in seronegative individuals after both vaccination and asymptomatic infection (omicron variant). T cell responses are reported from only one of the four site cohorts where the vaccination schedule preceded the omicron wave. In seronegative individuals, Covishield™ elicited both CD4+ and CD8+ spike-specific cytokine-producing T cells whereas Covaxin® elicited mainly CD4+ spike-specific T cells. Neither vaccine showed significant post-vaccination expansion of spike-specific T cells in seropositive individuals.
INTERPRETATION
Covishield™ elicited immune responses of higher magnitude and breadth than Covaxin® in both seronegative individuals and seropositive individuals, across cohorts representing the pre-vaccination immune history of most of the vaccinated Indian population.
FUNDING
Corporate social responsibility (CSR) funding from Hindustan Unilever Limited (HUL) and Unilever India Pvt. Ltd. (UIPL).
背景
全球范围内,关于疫苗平台在体液免疫和细胞免疫反应方面的头对头比较、并按接种前血清状态分层的数据有限。印度18至45岁人群的新冠疫苗接种工作于2021年4月开始,当时由于2021年4月至5月新冠疫情的德尔塔浪潮,普通人群的血清阳性率正在上升。
方法
2021年6月30日至2022年1月28日期间,我们在印度的四个临床地点招募了691名18至45岁的参与者。在这项非随机且实验室盲法研究中,参与者根据国家疫苗接种政策,分别接种两剂Covaxin®(间隔4周)或两剂Covishield™(间隔12周)。主要结局是两剂疫苗接种后针对严重急性呼吸综合征冠状病毒2(SARS-CoV-2)刺突蛋白和核衣壳蛋白的血清转化率和抗体几何平均滴度(GMT)。次要结局是接种疫苗前后细胞免疫反应的频率。
研究结果
与接种前基线相比,两种疫苗在血清阴性和血清阳性个体中均引发了具有统计学意义的血清转化和结合抗体水平。在符合方案队列中,就血清转化率(血清阴性个体中为98.3%对74.4%,p<0.0001;血清阳性个体中为91.7%对66.9%,p<0.0001)以及针对原始毒株的抗刺突抗体水平(血清阴性个体中GMT为1272.1对75.4结合抗体单位/毫升[BAU/ml],p<0.0001;血清阳性个体中为2089.07对585.7 BAU/ml,p<0.0001)而言,Covishield™引发的抗体反应高于Covaxin®。由于并非所有临床地点的参与者都在同一时间招募,特定地点的免疫原性受到相对于德尔塔和奥密克戎浪潮的疫苗接种时间的影响。Covishield™接种者针对包括德尔塔和奥密克戎在内的关注变异株的替代中和抗体反应高于Covaxin®接种者;在接种疫苗和无症状感染(奥密克戎变异株)后,血清阳性个体中的反应高于血清阴性个体。仅在四个地点队列中的一个报告了T细胞反应,该队列的疫苗接种时间表早于奥密克戎浪潮。在血清阴性个体中,Covishield™引发了CD4+和CD8+刺突特异性细胞因子产生T细胞,而Covaxin®主要引发了CD4+刺突特异性T细胞。两种疫苗在血清阳性个体中均未显示出接种后刺突特异性T细胞的显著扩增。
解读
在代表大多数已接种疫苗的印度人群接种前免疫史的队列中,Covishield™在血清阴性个体和血清阳性个体中引发的免疫反应在强度和广度上均高于Covaxin®。
资金来源
来自印度斯坦联合利华有限公司(HUL)和联合利华印度私人有限公司(UIPL)公司社会责任(CSR)资金。
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